静脉注射人羊膜上皮细胞联合组织型纤溶酶原激活剂对缺血性中风后脑损伤的保护作用。
Protection against brain injury after ischemic stroke by intravenous human amnion epithelial cells in combination with tissue plasminogen activator.
作者信息
Barreto-Arce Liz J, Kim Hyun Ah, Chan Siow Teng, Lim Rebecca, Drummond Grant R, Ma Henry, Phan Thanh G, Sobey Christopher G, Zhang Shenpeng R
机构信息
Department of Microbiology, Anatomy, Physiology, and Pharmacology and Centre for Cardiovascular Biology and Disease Research, School of Agriculture, Biomedicine and Environment, La Trobe University, Bundoora, VIC, Australia.
The Ritchie Centre, Hudson Institute of Medical Research, Clayton, VIC, Australia.
出版信息
Front Neurosci. 2023 Jun 16;17:1157236. doi: 10.3389/fnins.2023.1157236. eCollection 2023.
BACKGROUND
Thrombolytic agents such as tissue plasminogen activator (tPA) are the only drug class approved to treat ischemic stroke and are usually administered within 4.5 h. However, only ~20% of ischemic stroke patients are eligible to receive the therapy. We previously demonstrated that early intravenous administration of human amnion epithelial cells (hAECs) can limit brain inflammation and infarct growth in experimental stroke. Here, we have tested whether hAECs exert cerebroprotective effects in combination with tPA in mice.
METHODS
Male C57Bl/6 mice were subjected to middle cerebral artery occlusion for 60 min followed by reperfusion. Immediately following reperfusion, vehicle (saline, = 31) or tPA (10 mg/kg; = 73) was administered intravenously. After 30 min of reperfusion, tPA-treated mice were injected intravenously with either hAECs (1×10; = 32) or vehicle (2% human serum albumin; = 41). A further 15 sham-operated mice were treated with vehicle ( = 7) or tPA + vehicle ( = 8). Mice were designated to be euthanised at 3, 6 or 24 h post-stroke ( = 21, 31, and 52, respectively), and brains were collected to assess infarct volume, blood-brain barrier (BBB) disruption, intracerebral bleeding and inflammatory cell content.
RESULTS
There was no mortality within 6 h of stroke onset, but a high mortality occurred in tPA + saline-treated mice between 6 h and 24 h post-stroke in comparison to mice treated with tPA + hAECs (61% vs. 27%, = 0.04). No mortality occurred within 24 h of sham surgery in mice treated with tPA + vehicle. We focused on early infarct expansion within 6 h of stroke and found that infarction was ~50% larger in tPA + saline- than in vehicle-treated mice (23 ± 3 mm vs. 15 ± 2 mm, = 0.02) but not in mice receiving tPA + hAECs (13 ± 2 mm, < 0.01 vs. tPA + saline) in which intracerebral hAECs were detected. Similar to the profiles of infarct expansion, BBB disruption and intracerebral bleeding in tPA + saline-treated mice at 6 h was 50-60% greater than in vehicle-treated controls (2.6 ± 0.5 vs. 1.6 ± 0.2, = 0.05) but not after tPA + hAECs treatment (1.7 ± 0.2, = 0.10 vs. tPA + saline). No differences in inflammatory cell content were detected between treatment groups.
CONCLUSION
When administered following tPA in acute stroke, hAECs improve safety and attenuate infarct growth in association with less BBB disruption and lower 24 h mortality.
背景
组织纤溶酶原激活剂(tPA)等溶栓药物是唯一被批准用于治疗缺血性中风的药物类别,通常在4.5小时内给药。然而,只有约20%的缺血性中风患者有资格接受该治疗。我们之前证明,早期静脉注射人羊膜上皮细胞(hAECs)可以限制实验性中风中的脑炎症和梗死灶扩大。在此,我们测试了hAECs与tPA联合应用在小鼠中是否发挥脑保护作用。
方法
雄性C57Bl/6小鼠接受大脑中动脉闭塞60分钟,随后再灌注。再灌注后立即静脉注射溶剂(生理盐水,n = 31)或tPA(10 mg/kg;n = 73)。再灌注30分钟后,tPA治疗的小鼠静脉注射hAECs(1×10;n = 32)或溶剂(2%人血清白蛋白;n = 41)。另外15只假手术小鼠接受溶剂(n = 7)或tPA + 溶剂(n = 8)治疗。小鼠在中风后3、6或24小时被指定安乐死(分别为n = 21、31和52),收集大脑以评估梗死体积、血脑屏障(BBB)破坏、脑内出血和炎症细胞含量。
结果
中风发作后6小时内无死亡,但与tPA + hAECs治疗的小鼠相比,tPA + 生理盐水治疗的小鼠在中风后6小时至24小时内死亡率较高(61%对27%,P = 0.04)。tPA + 溶剂治疗的小鼠在假手术后24小时内无死亡。我们关注中风后6小时内的早期梗死灶扩大,发现tPA + 生理盐水治疗的小鼠梗死面积比溶剂治疗的小鼠大约50%(23±3 mm对15±2 mm,P = 0.02),但接受tPA + hAECs治疗的小鼠(13±2 mm,与tPA + 生理盐水相比P < 0.01)未出现这种情况,其中检测到脑内有hAECs。与梗死灶扩大情况相似,tPA + 生理盐水治疗的小鼠在6小时时BBB破坏和脑内出血比溶剂治疗的对照组大(2.6±0.5对1.6±0.2,P = 0.05),但tPA + hAECs治疗后未出现这种情况(1.7±0.2,与tPA + 生理盐水相比P = 0.10)。各治疗组之间炎症细胞含量未检测到差异。
结论
在急性中风中tPA给药后再给予hAECs,可提高安全性,减轻梗死灶扩大,同时伴有较少的BBB破坏和较低的24小时死亡率。
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